| Literature DB >> 33533717 |
Emilie V Russler-Germain1, Jaeu Yi1, Shannon Young1, Katherine Nutsch1, Harikesh S Wong2, Teresa L Ai1, Jiani N Chai1, Vivek Durai3, Daniel H Kaplan4, Ronald N Germain2, Kenneth M Murphy3, Chyi-Song Hsieh1.
Abstract
Generation of tolerogenic peripheral regulatory T (pTreg) cells is commonly thought to involve CD103+ gut dendritic cells (DCs), yet their role in commensal-reactive pTreg development is unclear. Using two Helicobacter-specific T cell receptor (TCR) transgenic mouse lines, we found that both CD103+ and CD103- migratory, but not resident, DCs from the colon-draining mesenteric lymph node presented Helicobacter antigens to T cells ex vivo. Loss of most CD103+ migratory DCs in vivo using murine genetic models did not affect the frequency of Helicobacter-specific pTreg cell generation or induce compensatory tolerogenic changes in the remaining CD103- DCs. By contrast, activation in a Th1-promoting niche in vivo blocked Helicobacter-specific pTreg generation. Thus, these data suggest a model where DC-mediated effector T cell differentiation is 'dominant', necessitating that all DC subsets presenting antigen are permissive for pTreg cell induction to maintain gut tolerance.Entities:
Keywords: Helicobacter; colon; dendritic cell; immunology; inflammation; microbiota; mouse; regulatory t cell; tolerance
Mesh:
Year: 2021 PMID: 33533717 PMCID: PMC7877908 DOI: 10.7554/eLife.54792
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140